Immunopathogenesis of hidradenitis suppurativa and response to anti–TNF-α therapy
Margaret M. Lowe, … , Scott L. Hansen, Michael D. Rosenblum
Margaret M. Lowe, … , Scott L. Hansen, Michael D. Rosenblum
Published August 25, 2020
Citation Information: JCI Insight. 2020;5(19):e139932. https://doi.org/10.1172/jci.insight.139932.
View: Text | PDF | Corrigendum
Research Article Dermatology Immunology

Immunopathogenesis of hidradenitis suppurativa and response to anti–TNF-α therapy

Abstract

Hidradenitis suppurativa (HS) is a highly prevalent, morbid inflammatory skin disease with limited treatment options. The major cell types and inflammatory pathways in skin of patients with HS are poorly understood, and which patients will respond to TNF-α blockade is currently unknown. We discovered that clinically and histologically healthy appearing skin (i.e., nonlesional skin) is dysfunctional in patients with HS with a relative loss of immune regulatory pathways. HS skin lesions were characterized by quantitative and qualitative dysfunction of type 2 conventional dendritic cells, relatively reduced regulatory T cells, an influx of memory B cells, and a plasma cell/plasmablast infiltrate predominantly in end-stage fibrotic skin. At the molecular level, there was a relative bias toward the IL-1 pathway and type 1 T cell responses when compared with both healthy skin and psoriatic patient skin. Anti–TNF-α therapy markedly attenuated B cell activation with minimal effect on other inflammatory pathways. Finally, we identified an immune activation signature in skin before anti–TNF-α treatment that correlated with subsequent lack of response to this modality. Our results reveal the fundamental immunopathogenesis of HS and provide a molecular foundation for future studies focused on stratifying patients based on likelihood of clinical response to TNF-α blockade.

Authors

Margaret M. Lowe, Haley B. Naik, Sean Clancy, Mariela Pauli, Kathleen M. Smith, Yingtao Bi, Robert Dunstan, Johann E. Gudjonsson, Maia Paul, Hobart Harris, Esther Kim, Uk Sok Shin, Richard Ahn, Wilson Liao, Scott L. Hansen, Michael D. Rosenblum

×

Figure 1

Elucidation of the dominant inflammatory pathways in HS skin.

Options: View larger image (or click on image) Download as PowerPoint
Elucidation of the dominant inflammatory pathways in HS skin. (A) Princi...
(A) Principal components analysis (PCA) of whole-tissue RNA-Seq data from lesional HS skin (n = 19), nonlesional HS skin (n = 13), and site-matched healthy control skin (n = 16). All samples were taken before the initiation of anti–TNF-α therapy. (B) The top 20 enriched (FDR < 0.05, Fisher exact with Benjamini-Hochberg correction) PANTHER Gene Ontology pathways identified from genes significantly (adjusted P < 0.05, Wald’s test) increased in pretreatment lesional HS skin versus healthy control skin are depicted in red. Fold enrichment of pathways in genes significantly (adjusted P < 0.05, Wald’s test) increased in lesional psoriasis skin (n = 8) versus healthy control skin (n = 9) is depicted in blue. (C) Heatmap depicting the Gene Set Variation Analysis (GSVA) enrichment scores of the top 50 significantly different (adjusted P < 0.05, empirical Bayes test with Benjamini-Hochberg correction) Gene Ontology pathways in whole-tissue RNA-Seq data of pretreatment HS lesional skin versus healthy control skin. Each column depicts an individual patient. Average pathway enrichment scores in HS skin, normal skin, and psoriatic skin, is depicted (left); pathways significantly different (adjusted P < 0.05) comparing HS skin and psoriatic skin are indicated. (D) Ingenuity Pathway Analysis (IPA) of upstream regulators significantly (P < 0.05) different in lesional HS skin versus healthy controls. (E) xCell Scores indicating predicted enrichment of different cell populations in whole-tissue RNA-Seq data from lesional HS (L) and healthy (H) skin. Each dot represents an individual patient. All figure error bars show mean ± SEM. (**P < 0.01, ****P < 0.0001, Mann-Whitney U test.)